Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity

SB056 is a novel semi-synthetic antimicrobial peptide with a dimeric dendrimer scaffold. Active against both Gram-negative and -positive bacteria, its mechanism has been attributed to a disruption of bacterial membranes. The branched peptide was shown to assume a β-stranded conformation in a lipidic...

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Autores principales: Manzo, Giorgia, Scorciapino, Mariano A., Wadhwani, Parvesh, Bürck, Jochen, Montaldo, Nicola Pietro, Pintus, Manuela, Sanna, Roberta, Casu, Mariano, Giuliani, Andrea, Pirri, Giovanna, Luca, Vincenzo, Ulrich, Anne S., Rinaldi, Andrea C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4305290/
https://www.ncbi.nlm.nih.gov/pubmed/25617899
http://dx.doi.org/10.1371/journal.pone.0116379
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author Manzo, Giorgia
Scorciapino, Mariano A.
Wadhwani, Parvesh
Bürck, Jochen
Montaldo, Nicola Pietro
Pintus, Manuela
Sanna, Roberta
Casu, Mariano
Giuliani, Andrea
Pirri, Giovanna
Luca, Vincenzo
Ulrich, Anne S.
Rinaldi, Andrea C.
author_facet Manzo, Giorgia
Scorciapino, Mariano A.
Wadhwani, Parvesh
Bürck, Jochen
Montaldo, Nicola Pietro
Pintus, Manuela
Sanna, Roberta
Casu, Mariano
Giuliani, Andrea
Pirri, Giovanna
Luca, Vincenzo
Ulrich, Anne S.
Rinaldi, Andrea C.
author_sort Manzo, Giorgia
collection PubMed
description SB056 is a novel semi-synthetic antimicrobial peptide with a dimeric dendrimer scaffold. Active against both Gram-negative and -positive bacteria, its mechanism has been attributed to a disruption of bacterial membranes. The branched peptide was shown to assume a β-stranded conformation in a lipidic environment. Here, we report on a rational modification of the original, empirically derived linear peptide sequence [WKKIRVRLSA-NH(2), SB056-lin]. We interchanged the first two residues [KWKIRVRLSA-NH(2), β-SB056-lin] to enhance the amphipathic profile, in the hope that a more regular β-strand would lead to a better antimicrobial performance. MIC values confirmed that an enhanced amphiphilic profile indeed significantly increases activity against both Gram-positive and -negative strains. The membrane binding affinity of both peptides, measured by tryptophan fluorescence, increased with an increasing ratio of negatively charged/zwitterionic lipids. Remarkably, β-SB056-lin showed considerable binding even to purely zwitterionic membranes, unlike the original sequence, indicating that besides electrostatic attraction also the amphipathicity of the peptide structure plays a fundamental role in binding, by stabilizing the bound state. Synchrotron radiation circular dichroism and solid-state (19)F-NMR were used to characterize and compare the conformation and mobility of the membrane bound peptides. Both SB056-lin and β-SB056-lin adopt a β-stranded conformation upon binding POPC vesicles, but the former maintains an intrinsic structural disorder that also affects its aggregation tendency. Upon introducing some anionic POPG into the POPC matrix, the sequence-optimized β-SB056-lin forms well-ordered β-strands once electro-neutrality is approached, and it aggregates into more extended β-sheets as the concentration of anionic lipids in the bilayer is raised. The enhanced antimicrobial activity of the analogue correlates with the formation of these extended β-sheets, which also leads to a dramatic alteration of membrane integrity as shown by (31)P-NMR. These findings are generally relevant for the design and optimization of other membrane-active antimicrobial peptides that can fold into amphipathic β-strands.
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spelling pubmed-43052902015-01-30 Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity Manzo, Giorgia Scorciapino, Mariano A. Wadhwani, Parvesh Bürck, Jochen Montaldo, Nicola Pietro Pintus, Manuela Sanna, Roberta Casu, Mariano Giuliani, Andrea Pirri, Giovanna Luca, Vincenzo Ulrich, Anne S. Rinaldi, Andrea C. PLoS One Research Article SB056 is a novel semi-synthetic antimicrobial peptide with a dimeric dendrimer scaffold. Active against both Gram-negative and -positive bacteria, its mechanism has been attributed to a disruption of bacterial membranes. The branched peptide was shown to assume a β-stranded conformation in a lipidic environment. Here, we report on a rational modification of the original, empirically derived linear peptide sequence [WKKIRVRLSA-NH(2), SB056-lin]. We interchanged the first two residues [KWKIRVRLSA-NH(2), β-SB056-lin] to enhance the amphipathic profile, in the hope that a more regular β-strand would lead to a better antimicrobial performance. MIC values confirmed that an enhanced amphiphilic profile indeed significantly increases activity against both Gram-positive and -negative strains. The membrane binding affinity of both peptides, measured by tryptophan fluorescence, increased with an increasing ratio of negatively charged/zwitterionic lipids. Remarkably, β-SB056-lin showed considerable binding even to purely zwitterionic membranes, unlike the original sequence, indicating that besides electrostatic attraction also the amphipathicity of the peptide structure plays a fundamental role in binding, by stabilizing the bound state. Synchrotron radiation circular dichroism and solid-state (19)F-NMR were used to characterize and compare the conformation and mobility of the membrane bound peptides. Both SB056-lin and β-SB056-lin adopt a β-stranded conformation upon binding POPC vesicles, but the former maintains an intrinsic structural disorder that also affects its aggregation tendency. Upon introducing some anionic POPG into the POPC matrix, the sequence-optimized β-SB056-lin forms well-ordered β-strands once electro-neutrality is approached, and it aggregates into more extended β-sheets as the concentration of anionic lipids in the bilayer is raised. The enhanced antimicrobial activity of the analogue correlates with the formation of these extended β-sheets, which also leads to a dramatic alteration of membrane integrity as shown by (31)P-NMR. These findings are generally relevant for the design and optimization of other membrane-active antimicrobial peptides that can fold into amphipathic β-strands. Public Library of Science 2015-01-24 /pmc/articles/PMC4305290/ /pubmed/25617899 http://dx.doi.org/10.1371/journal.pone.0116379 Text en © 2015 Manzo et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Manzo, Giorgia
Scorciapino, Mariano A.
Wadhwani, Parvesh
Bürck, Jochen
Montaldo, Nicola Pietro
Pintus, Manuela
Sanna, Roberta
Casu, Mariano
Giuliani, Andrea
Pirri, Giovanna
Luca, Vincenzo
Ulrich, Anne S.
Rinaldi, Andrea C.
Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity
title Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity
title_full Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity
title_fullStr Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity
title_full_unstemmed Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity
title_short Enhanced Amphiphilic Profile of a Short β-Stranded Peptide Improves Its Antimicrobial Activity
title_sort enhanced amphiphilic profile of a short β-stranded peptide improves its antimicrobial activity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4305290/
https://www.ncbi.nlm.nih.gov/pubmed/25617899
http://dx.doi.org/10.1371/journal.pone.0116379
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